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用于抗癌过继性T细胞治疗的CD8 T细胞的体外短时间白细胞介素-12预处理

Brief in vitro IL-12 conditioning of CD8 T Cells for anticancer adoptive T cell therapy.

作者信息

Salem Mohamed Labib, Salman Samar, Barnawi Ibrahim O

机构信息

Immunology and Biotechnology Unit, Zoology Department, Faculty of Science, Tanta University, Tanta, Egypt.

Center of Excellence in Cancer Research (CECR), Tanta University, Tanta, Egypt.

出版信息

Cancer Immunol Immunother. 2021 Oct;70(10):2751-2759. doi: 10.1007/s00262-021-02887-7. Epub 2021 May 8.

DOI:10.1007/s00262-021-02887-7
PMID:33966093
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10992799/
Abstract

Cancer immunotherapy represents a potential treatment approach through non-specific and specific enhancement of the immune responses. Adoptive cell therapy (ACT) is a potential modality of immunotherapy that depends on harvesting T cells from the tumor-bearing host, activating them in vitro and infusing them back to the same host. Several cytokines, in particular IL-2, IL-7 and IL-15, have been used to enhance survival T cells in vitro. Although effective, conditioning of T cells in vitro with these cytokines requires long-term culture which results in the loss of expression of their trafficking receptors mainly CD62L. It also results in exhaustion of the activated T cells and reduction in their functions upon adoptive transfer in vivo. Our recent studies and those of other groups showed that brief (3 days) conditioning of CD8 T cells by IL-12 in vitro can result in enhancing function of tumor-reactive CD8 T cells. Adoptive transfer of these IL-12-conditioned CD8 T cells into tumor-bearing mice, preconditioned with cyclophosphamide, 1 day before ACT, induced tumor eradication that was associated with generation of tumor-specific memory response. In this review, we summarize studies that indicated to the superiority of IL-12 as a potential cytokine for conditioning T cells for ACT. In addition, we discuss some of the cellular and molecular mechanisms that govern how IL-12 programs CD8 T cells to enhance their functionality especially in vitro and its implication in combination with other ACT modalities, opening a avenue for the clinical application of this cytokine.

摘要

癌症免疫疗法是一种通过非特异性和特异性增强免疫反应来实现的潜在治疗方法。过继性细胞疗法(ACT)是免疫疗法的一种潜在形式,它依赖于从荷瘤宿主中采集T细胞,在体外激活它们,然后再回输到同一宿主中。几种细胞因子,特别是白细胞介素-2(IL-2)、白细胞介素-7(IL-7)和白细胞介素-15(IL-15),已被用于在体外增强存活T细胞。尽管有效,但用这些细胞因子在体外对T细胞进行预处理需要长期培养,这会导致其主要运输受体CD62L的表达丧失。这也会导致活化T细胞耗竭,并在体内过继转移后其功能降低。我们最近的研究以及其他团队的研究表明,体外使用IL-12对CD8 T细胞进行短暂(3天)预处理可增强肿瘤反应性CD8 T细胞的功能。在ACT前1天,将这些经IL-12预处理的CD8 T细胞过继转移到用环磷酰胺预处理的荷瘤小鼠中,可诱导肿瘤根除,这与肿瘤特异性记忆反应的产生有关。在这篇综述中,我们总结了表明IL-12作为一种潜在的细胞因子在预处理T细胞用于ACT方面具有优越性的研究。此外,我们还讨论了一些细胞和分子机制,这些机制决定了IL-12如何编程CD8 T细胞以增强其功能,特别是在体外,以及它与其他ACT模式联合使用的意义,为这种细胞因子的临床应用开辟了一条道路。

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Stem-like CD8 T cells mediate response of adoptive cell immunotherapy against human cancer.类干细胞 CD8 T 细胞介导过继性细胞免疫疗法对人类癌症的反应。
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